Effects of quetiapine treatment on cocaine self-administration and behavioral indices of sleep in adult rhesus monkeys

Brutcher, Robert E.; Nader, Michael A.

doi:10.1007/s00213-014-3672-5

Cited by 11 publications

(8 citation statements)

References 52 publications

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“…In agreement with these clinical results, subchronic treatment with the DA D2 antagonists flupenthixol, haloperidol, chlorpromazine, and quetiapine did not decrease and sometimes increased cocaine choice [22, 58, 59]. Consistent with these published results, subchronic treatment with DA antagonist risperidone also failed to attenuate cocaine vs. food choice (Hutsell, Negus, and Banks, unpublished observations).…”

Section: Evaluation Of Candidate Medications In Preclinical Drug Vs supporting

confidence: 73%

Use of Preclinical Drug Vs. Food Choice Procedures to Evaluate Candidate Medications for Cocaine Addiction

Banks

Hutsell

Schwienteck

et al. 2015

Curr Treat Options Psych

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Opinion Statement Drug addiction is a disease that manifests as an inappropriate allocation of behavior towards the procurement and use of the abused substance and away from other behaviors that produce more adaptive reinforcers (e.g. exercise, work, family and social relationships). The goal of treating drug addiction is not only to decrease drug-maintained behaviors, but also to promote a reallocation of behavior towards alternative, nondrug reinforcers. Experimental procedures that offer concurrent access to both a drug reinforcer and an alternative, nondrug reinforcer provide a research tool for assessment of medication effects on drug choice and behavioral allocation. Choice procedures are currently the standard in human laboratory research on medications development. Preclinical choice procedures have been utilized in biomedical research since the early 1940’s, and during the last 10–15 years, their use for evaluation of medications to treat drug addiction has increased. We propose here that parallel use of choice procedures in preclinical and clinical studies will facilitate translational research on development of medications to treat cocaine addiction. In support of this proposition, a review of the literature suggests strong concordance between preclinical effectiveness of candidate medications to modify cocaine choice in nonhuman primates and rodents and clinical effectiveness of these medications to modify either cocaine choice in human laboratory studies or metrics of cocaine abuse in patients with cocaine use disorder. The strongest evidence for medication effectiveness in preclinical choice studies has been obtained with maintenance on the monoamine releaser d-amphetamine, a candidate agonist medication for cocaine use analogous to use of methadone to treat heroin abuse or nicotine formulations to treat tobacco dependence.

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Section: Evaluation Of Candidate Medications In Preclinical Drug Vs supporting

confidence: 73%

Use of Preclinical Drug Vs. Food Choice Procedures to Evaluate Candidate Medications for Cocaine Addiction

Banks

Hutsell

Schwienteck

et al. 2015

Curr Treat Options Psych

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“…The reason a receptor antagonist would increase low-dose cocaine choice over food is not known. The present findings replicate earlier results using cocainefood choice (Brutcher and Nader, 2015), where oral quetiapine did not affect cocaine choice when preferred (i.e., .80% choice) cocaine doses were available for self-administration. These data appear in contrast to the findings in psychiatric patients in which quetiapine treatment decreased cocaine/amphetamine craving (Brown et al, 2003), although the latter findings required up to 5 weeks of treatment, and dollars spent on drugs (i.e., actual self-administration) were not affected by quetiapine treatment.…”

Section: Discussionsupporting

confidence: 89%

“…The first treatment occurred at approximately 0730 (90 minutes prior to the experimental session) and the second treatment at approximately 1700. This quetiapine dose was chosen as the minimally disruptive dose in male monkeys (Brutcher and Nader, 2015). During the first 4 weeks of treatment, only food-maintained responding was examined, after which saline and the quetiapine dose-response curve was redetermined as described earlier; oral quetiapine treatment continued throughout the redetermination of the self-administration dose-response curve.…”

Section: Methodsmentioning

confidence: 99%

Evaluation of the Reinforcing Effect of Quetiapine, Alone and in Combination with Cocaine, in Rhesus Monkeys

Brutcher

Nader

2015

Journal of Pharmacology and Experimental Therapeutics

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There are several case reports of nonmedicinal quetiapine abuse, yet there are very limited preclinical studies investigating quetiapine self-administration. The goal of this study was to investigate the reinforcing effects of quetiapine alone and in combination with intravenous cocaine in monkeys. In experiment 1, cocaine-experienced female monkeys (N 5 4) responded under a fixed-ratio (FR) 30 schedule of food reinforcement (1.0-g banana-flavored pellets), and when responding was stable, quetiapine (0.003-0.1 mg/kg per injection) or saline was substituted for a minimum of five sessions; there was a return to food-maintained responding between doses. Next, monkeys were treated with quetiapine (25 mg, by mouth, twice a day) for approximately 30 days, and then the quetiapine selfadministration dose-response curve was redetermined. In experiment 2, male monkeys (N 5 6) self-administered cocaine under a concurrent FR schedule with food reinforcement (three food pellets) as the alternative to cocaine (0.003-0.3 mg/kg per injection) presentation. Once choice responding was stable, the effects of adding quetiapine (0.03 or 0.1 mg/kg per injection) to the cocaine solution were examined. In experiment 1, quetiapine did not function as a reinforcer, and chronic quetiapine treatment did not alter these effects. In experiment 2, cocaine choice increased in a dose-dependent fashion. The addition of quetiapine to cocaine resulted in increases in lowdose cocaine choice and number of cocaine injections in four monkeys, while not affecting high-dose cocaine preference. Thus, although quetiapine alone does not have abuse potential, there was evidence of enhancement of the reinforcing potency of cocaine. These results suggest that the use of quetiapine in cocaine-addicted patients should be monitored.

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“…Non-human animal studies, conducted primarily in rhesus monkeys but also in rats, have tested the following medications while specifically using drug-choice procedures: aripiprazole (Thomsen et al, 2008), buspirone (John et al, 2015), d-amphetamine (Negus, 2003; Thomsen et al, 2013; Banks et al, 2015b), fenfluramine (Banks et al, 2011), fluoroamphetamine (Banks et al, 2011), flupenthixol (Negus, 2003), lisdexamfetamine (Banks et al, 2015b), methadone (Negus and Mello, 2004), methamphetamine (Banks et al, 2011), napthylisopropylamine (Banks et al, 2011), phendimetrazine (Banks et al, 2013c; Banks et al, 2013a), phenmetrazine (Banks et al, 2011, 2013b), quetiapine (Brutcher and Nader, 2015), and xanomeline (Thomsen et al, 2014). In general, drugs that could be considered “agonist replacement” medications like d-amphetamine, lisdexamfetamine, phendimetrazine, and phenmetrazine reduced cocaine choice (Negus, 2003; Banks et al, 2013c; Banks et al, 2013b, a; Thomsen et al, 2013; Banks et al, 2015b).…”

Section: Preclinical and Human Laboratory Choice Study Outcomesmentioning

confidence: 99%

“…In general, drugs that could be considered “agonist replacement” medications like d-amphetamine, lisdexamfetamine, phendimetrazine, and phenmetrazine reduced cocaine choice (Negus, 2003; Banks et al, 2013c; Banks et al, 2013b, a; Thomsen et al, 2013; Banks et al, 2015b). Antagonist-type pharmacotherapies, conversely, either failed to decrease cocaine choice [e.g., buspirone, flupenthixol or methadone (Negus, 2003; Negus and Mello, 2004; John et al, 2015)] or produced only transient decreases in cocaine choice [e.g., quetiapine or aripiprazole (Thomsen et al, 2008; Brutcher and Nader, 2015)]. Xanomeline, a muscarinic M1/M4 receptor agonist, decreased cocaine choice and was not associated with tolerance in rats (Thomsen et al, 2014).…”

Section: Preclinical and Human Laboratory Choice Study Outcomesmentioning

confidence: 99%

Cocaine choice procedures in animals, humans, and treatment-seekers: Can we bridge the divide?

Moeller

Stoops

2015

Pharmacology Biochemistry and Behavior

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Individuals with cocaine use disorder chronically self-administer cocaine to the detriment of other rewarding activities, a phenomenon best modeled in laboratory drug-choice procedures. These procedures can evaluate the reinforcing effects of drugs versus comparably valuable alternatives under multiple behavioral arrangements and schedules of reinforcement. However, assessing drug-choice in treatment-seeking or abstaining humans poses unique challenges: for ethical reasons, these populations typically cannot receive active drugs during research studies. Researchers have thus needed to rely on alternative approaches that approximate drug-choice behavior or assess more general forms of decision-making, but whether these alternatives have relevance to real-world drug-taking that can inform clinical trials is not well-understood. In this mini-review, we (A) summarize several important modulatory variables that influence cocaine choice in nonhuman animals and non-treatment seeking humans; (B) discuss some of the ethical considerations that could arise if treatment-seekers are enrolled in drug-choice studies; (C) consider the efficacy of alternative procedures, including non-drug-related decision-making and ‘simulated’ drug-choice (a choice is made, but no drug is administered) to approximate drug choice; and (D) suggest opportunities for new translational work to bridge the current divide between preclinical and clinical research.

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Effects of quetiapine treatment on cocaine self-administration and behavioral indices of sleep in adult rhesus monkeys

Cited by 11 publications

References 52 publications

Use of Preclinical Drug Vs. Food Choice Procedures to Evaluate Candidate Medications for Cocaine Addiction

Use of Preclinical Drug Vs. Food Choice Procedures to Evaluate Candidate Medications for Cocaine Addiction

Evaluation of the Reinforcing Effect of Quetiapine, Alone and in Combination with Cocaine, in Rhesus Monkeys

Cocaine choice procedures in animals, humans, and treatment-seekers: Can we bridge the divide?

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